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Reconstruction of the Mouse Otocyst and Early Neuroblast Lineage at Single-Cell Resolution

机译:以单细胞分辨率重建小鼠耳囊和早期成神经细胞谱系。

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摘要

The otocyst harbors progenitors for most cell types of the mature inner ear. Developmental lineage analyses and gene expression studies suggest that distinct progenitor populations are compartmentalized to discrete axial domains in the early otocyst. Here, we conducted highly parallel quantitative RT-PCR measurements on 382 individual cells from the developing otocyst and neuroblast lineages to assay 96 genes representing established otic markers, signaling-pathway-associated transcripts, and novel otic-specific genes. By applying multivariate cluster, principal component, and network analyses to the data matrix, we were able to readily distinguish the delaminating neuroblasts and to describe progressive states of gene expression in this population at single-cell resolution. It further established a three-dimensional model of the otocyst in which each individual cell can be precisely mapped into spatial expression domains. Our bioinformatic modeling revealed spatial dynamics of different signaling pathways active during early neuroblast development and prosensory domain specification.
机译:耳囊具有成熟内耳大多数细胞类型的祖细胞。发育谱系分析和基因表达研究表明,不同的祖细胞群在早期的囊肿中被分隔成离散的轴向结构域。在这里,我们对来自发育中的囊胚和成神经细胞谱系的382个单个细胞进行了高度并行的定量RT-PCR测量,以测定代表已建立的耳标志物,信号通路相关转录本和新的耳特异性基因的96个基因。通过将多元聚类,主成分和网络分析应用于数据矩阵,我们能够轻松地区分分层的成神经细胞,并以单细胞分辨率描述该群体中基因表达的进展状态。它进一步建立了耳囊的三维模型,其中每个单个细胞都可以精确地映射到空间表达域中。我们的生物信息学模型揭示了在早期成神经细胞发育和prosensory域规范活跃的不同信号通路的空间动力学。

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